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A new soy germ fermented ingredient displays estrogenic and protease inhibitor activities able to prevent irritable bowel syndrome-like symptoms in stressed female rats

机译:一种新的大豆胚芽发酵成分具有雌激素和蛋白酶抑制剂活性,能够预防应激雌性大鼠肠易激综合征样症状

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Background and aims: Irritable Bowel syndrome (IBS) often associated with psychological distress, is characterized by increased gut permeability and visceral sensitivity. In animals, stress increases intestinal paracellular permeability (IPP), visceral sensitivity and colonic proteolytic activity. Estradiol reduces IPP and affects visceral sensitivity in non-stressed ovariectomized rats, but whether estrogens affect stress-induced hyperpermeability and hypersensitivity in cyclic females remains unclear. We aimed to evaluate (i) the effects of a phytoestrogen-rich soy germ fermented ingredient (SG) on visceral hypersensitivity, hyperpermeability and other symptoms in stressed intact female rats, (ii) the mechanisms of action involved on the basis of both estrogenic and protease inhibitor activities of SG. Methods: Female rats received orally for 15-d either SG, 17β-estradiol benzoate (EB), or vehicles, with or without the estrogen receptor (ER) antagonist ICI182.780 before stress. Visceral sensitivity, IPP, faecal proteolytic activity, plasma corticosterone, rat mast cell protease II immunostaining, and occludin expression were assessed. Results: Stress increased IPP (concomitantly to a drop in occludin expression), visceral sensitivity, faecal proteolytic activity and plasma corticosterone. Similarly to EB, SG prevented the stress-induced hyperpermeability, and hypersensitivity, without changes in plasma corticosterone. SG inhibited the increase in faecal proteolytic activity, enhanced occludin expression, and reduced the colonic mast cell density. All SG effects, except decrease on faecal proteolytic activity, were blocked by ICI182.780. Conclusion: A 2-wk oral treatment with SG prevented the stress-induced hyperpermeability and visceral hypersensitivity in cyclic rats through ER activation, and blocked the increase in colonic proteolytic activity, suggesting that SG can be promising in IBS management.
机译:背景与目的:肠易激综合征(IBS)通常与心理困扰有关,其特点是肠道通透性和内脏敏感性增加。在动物中,压力会增加肠道副细胞通透性(IPP),内脏敏感性和结肠蛋白水解活性。雌二醇可降低非应激卵巢切除大鼠的IPP并影响其内脏敏感性,但尚不清楚雌激素是否影响应激诱导的周期性雌性的通透性和超敏性。我们旨在评估(i)富含植物雌激素的大豆发酵成分(SG)对应激的完整雌性大鼠内脏超敏性,通透性及其他症状的影响,(ii)基于雌激素和雌激素的作用机理SG的蛋白酶抑制剂活性。方法:雌性大鼠在应激前口服SG,17β-雌二醇苯甲酸酯(EB)或赋形剂15天,含或不含雌激素受体(ER)拮抗剂ICI182.780。评估内脏敏感性,IPP,粪便蛋白水解活性,血浆皮质酮,大鼠肥大细胞蛋白酶II免疫染色和occludin表达。结果:压力增加IPP(伴随闭合蛋白表达下降),内脏敏感性,粪便蛋白水解活性和血浆皮质酮。与EB相似,SG可以防止压力诱导的通透性和超敏性,而血浆皮质类固醇没有变化。 SG抑制了粪便蛋白水解活性的增加,增强了occludin的表达,并降低了结肠肥大细胞的密度。除降低粪便蛋白水解活性外,所有SG作用均被ICI182.780阻断。结论:SG的2周口服治疗可通过ER激活来防止应激诱导的周期性大鼠过度通透性和内脏超敏性,并阻止结肠蛋白水解活性的增加,这表明SG在IBS的管理中可能是有希望的。

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